Bicarbonate correction of ketoacidosis alters host-pathogen interactions and alleviates mucormycosis
Teclegiorgis Gebremariam, … , Scott G. Filler, Ashraf S. Ibrahim
Teclegiorgis Gebremariam, … , Scott G. Filler, Ashraf S. Ibrahim
Published May 9, 2016
Citation Information: J Clin Invest. 2016;126(6):2280-2294. https://doi.org/10.1172/JCI82744.
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Research Article Infectious disease

Bicarbonate correction of ketoacidosis alters host-pathogen interactions and alleviates mucormycosis

Abstract

Patients with diabetic ketoacidosis (DKA) are uniquely predisposed to mucormycosis, an angioinvasive fungal infection with high mortality. Previously, we demonstrated that Rhizopus invades the endothelium via binding of fungal CotH proteins to the host receptor GRP78. Here, we report that surface expression of GRP78 is increased in endothelial cells exposed to physiological concentrations of β-hydroxy butyrate (BHB), glucose, and iron that are similar to those found in DKA patients. Additionally, expression of R. oryzae CotH was increased within hours of incubation with DKA-associated concentrations of BHB, glucose, and iron, augmenting the ability of R. oryzae to invade and subsequently damage endothelial cells in vitro. BHB exposure also increased fungal growth and attenuated R. oryzae neutrophil-mediated damage. Further, mice given BHB developed clinical acidosis and became extremely susceptible to mucormycosis, but not aspergillosis, while sodium bicarbonate reversed this susceptibility. BHB-related acidosis exerted a direct effect on both GRP78 and CotH expression, an effect not seen with lactic acidosis. However, BHB also indirectly compromised the ability of transferrin to chelate iron, as iron chelation combined with sodium bicarbonate completely protected endothelial cells from Rhizopus-mediated invasion and damage. Our results dissect the pathogenesis of mucormycosis during ketoacidosis and reinforce the importance of careful metabolic control of the acidosis to prevent and manage this infection.

Authors

Teclegiorgis Gebremariam, Lin Lin, Mingfu Liu, Dimitrios P. Kontoyiannis, Samuel French, John E. Edwards Jr., Scott G. Filler, Ashraf S. Ibrahim

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Figure 10

An illustration showing the proposed mechanism of susceptibility of the ketoacidotic host to mucormycosis.

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An illustration showing the proposed mechanism of susceptibility of the ...
Acidosis promotes the release of iron from transferrin (T) by protonation of the milieu. Released iron, elevated glucose, and ketone bodies (e.g., BHB) enhance the growth of the invading fungus as well as the surface expression of endothelial cell GRP78 and the fungal CotH proteins. The enhanced expression of the GRP78 receptor and its fungal ligand leads to increased invasion and subsequent injury to endothelial cells especially in the absence of neutrophil (PMN) killing of the invading fungus due to a detrimental effect exerted by iron and BHB on the phagocytes. This increased invasion results in hematogenous dissemination and organ seeding. NaHCO3 can reverse the effect of acidosis but not the direct effect of glucose, free iron, and BHB.